Geographic tongue and psoriasis: clinical, histopathological, immunohistochemical and genetic correlation - a literature review

Abstract: Geographic tongue is a chronic, inflammatory, and immune-mediated oral lesion of unknown etiology. It is characterized by serpiginous white areas around the atrophic mucosa, which alternation between activity, remission and reactivation at various locations gave the names benign migratory glossitis and wandering rash of the tongue. Psoriasis is a chronic inflammatory disease with frequent cutaneous involvement and an immunogenetic basis of great importance in clinical practice. The association between geographic tongue and psoriasis has been demonstrated in various studies, based on observation of its fundamental lesions, microscopic similarity between the two conditions and the presence of a common genetic marker, human leukocyte antigen (HLA) HLA-C*06. The difficulty however in accepting the diagnosis of geographic tongue as oral psoriasis is the fact that not all patients with geographic tongue present psoriasis. Some authors believe that the prevalence of geographic tongue would be much greater if psoriatic patients underwent thorough oral examination. This study aimed to develop a literature review performed between 1980 and 2014, in which consultation of theses, dissertations and selected scientific articles were conducted through search in Scielo and Bireme databases, from Medline and Lilacs sources, relating the common characteristics between geographic tongue and psoriasis. We observed that the frequency of oral lesions is relatively common, but to establish a correct diagnosis of oral psoriasis, immunohistochemical and genetic histopathological analyzes are necessary, thus highlighting the importance of oral examination in psoriatic patients and cutaneous examination in patients with geographic tongue.

Validez diagnóstica de antígenos leucocitarios humanos para el diagnóstico de la enfermedad de Behcet / Diagnostic validity of human leukocyte antigens for the diagnosis of Behcet's disease

INTRODUCCIÓN: La enfermedad de Behcet (EB) es una vasculitis sistémica de etiología desconocida, caracterizada por ulceraciones orales y genitales recurrentes asociadas y compromiso ocular. En la actualidad, el diagnóstico se realiza por medio de grupos de criterios diagnósticos. Aunque existe una asociación entre HLA-B51 y EB, no se ha considerado aún el uso de los HLA como prueba diagnóstica. OBJETIVO: Evaluar si existe un papel para los antígenos leucocitarios humanos, en particular los denominados HLA 15, 108, 105, 109 y 119, en el diagnóstico de pacientes con EB. MÉTODOS: Se realizó una búsqueda de revisiones sistemáticas de estudios de validez diagnóstica publicadas en los últimos cinco años en Cochrane Database of Systematic Reviews, DARE y MEDLINE, así como una búsqueda de estudios primarios sobre validez diagnóstica en MEDLINE (1966 a la fecha), EMBASE (1982 a la fecha), LILACS (1982 a la fecha), de referencias entre los estudios encontrados y consulta a expertos temáticos, productores y comercializadores de la tecnología; la tecnología de interés fue el uso de HLA para el diagnóstico de EB; como estándar de referencia se consideraron diferentes criterios clínicos (International Study Group (ISG), International Criteria For Behcet Disease (ICBD), entre otros). Dos evaluadores de manera independiente, tamizaron las referencias obtenidas, resolviendo las discrepancias por medio de un tercer autor. RESULTADOS: No es posible establecer conclusiones acerca del papel de los antígenos leucocitarios humanos en el diagnóstico de EB dado que, hasta la fecha, no se han publicado estudios sobre sus características operativas. En Colombia se requieren estimaciones de la frecuencia de alelos HLA y su asociación con EB que puedan sugerir su posible valor diagnóstico.(AU)

Dengue HLA associations in jamaicans / Asociaciones del HLA con el dengue en los jamaicanos

BACKGROUND: Polymorphisms in the human leukocyte antigen (HLA) genes might predispose certain individuals to dengue fever (DF) and the severe forms of the disease: dengue haemorrhagic fever/ dengue shock syndrome (DHF/DSS). SUBJECTS AND METHOD: A DNA-based HLA typing method was used to determine the HLA class I and II alleles in 50 patients with dengue, including 45 cases of DF, 5 cases of DHF and 177 healthy individuals in Jamaica. RESULTS: HLA -A*24 and -DR β5*01/02 were significantly associated with dengue infection while possession of HLA -A*23, - CW*04, -DQ β1*02, -DQ β1*03 and DQ β1*06 were protective. No other significant associations were found after correction for the number of alleles tested at each HLA - locus. CONCLUSION: This is the first study to report a significant association with HLA -A*24 and DF although this allele is associated with DHF and DSS in Vietnamese patients. The other HLA associations observed in the Jamaican cohort also are different from those reported in other ethnic groups. Further studies which involve larger numbers of patients with DHF and explore functional aspects of HLA allelic associations with dengue in Jamaicans are necessary.

ANTECEDENTES: Los polimorfismos de los genes del antígeno leucocitario humano (HLA) podría predisponer a ciertos individuos a la fiebre de dengue (FD) y a las formas severas de esta enfermedad: la fiebre hemorrágica de dengue y el síndrome de choque por dengue (FHD/SCD). SUJETOS Y MÉTODO: Se usó un método de tipificación HLA basado en el ADN con el propósito de determinar los alelos HLA clase I y II en 50 pacientes con dengue, incluyendo 45 casos de FD, 5 casos de FHD y 177 individuos saludables en Jamaica. RESULTADOS: HLA -A*24 y -DR β5*01/02 estuvieron significativamente asociados con la infección de dengue en tanto que la posesión de HLA -A*23, -CW*04, -DQ β1*02, -DQ β1*03 y DQ β1*06 tenía carácter protector. No se halló ninguna otra asociación significativa tras la corrección en relación con el número de alelos probados en cada locus de HLA . CONCLUSIÓN: Este es el primer estudio que reporta una asociación significativa de HLA -A*24 y FD, aunque este alelo se halla asociado con FHD y SCD en pacientes vietnamitas. Las otras asociaciones observadas en la cohorte jamaicana son también diferentes de las que se reportan para otros grupos étnicos. Se requieren estudios ulteriores que comprendan grandes números de pacientes con FHD y exploren los aspectos funcionales de las asociaciones alélicas de HLA con el dengue en los jamaicanos.

Seleção de doador de medula óssea ou sangue periférico / Bone marrow or peripheral blood donor selection

A compatibilidade HLA é o fator mais valorizado na escolha do doador de medula óssea voluntário, preconizando-se a realização de HLA de alta resolução nos locos HLA-A,B,C, DRB1 e DQB1. Tem sido dado preferência para o doador com consanguinidade alélica 8x8 (A,B,C, DRB1). Na presença de incompatibilidade na classe-I sugere-se a busca de doador com compatibilidade DQB1 (9x10). Já as incompatibilidades dos locos DPB1 não constituem critério de exclusão de doador, exceto quando existir presença de anticorpo contra o loco HLA-DP do doador.

The HLA system is considered the most important factor in choosing a volunteer bone marrow donor with the recommendation of performing high resolution HLA tests for the HLA-A, B, C, DRB1 and DQB1 loci. A preference has been given for donor 8x8 (A, B, C, DRB1) allele matching. In the presence of class-I incompatibility a search for DQB1 (9x10) donor compatibility is suggested. The incompatibility of the DPB1 locus does not constitute exclusion of the donor, except when there is the presence of antibodies against the HLA-DP locus of the donor.

Tipificación molecular de los antígenos leucocitarios humanos, estado del arte y perspectivas para los transplantes de células madre en Costa Rica: [revisión] / Molecular typing of human leukocyte antigens, state of the art and perspectives for stem cell transplantation in Costa Rica: [review]

El sistema de antígenos leucocitarios (human leukocyte antigen) es el más polimórfico en el ser humano. Su función la realiza regulando la respuesta inmune mediante su unión a moléculas como el receptor de células T, participando en la presentación de antígenos y el reconocimiento de lo propio en el organismo. Su papel central en la respuesta inmune así como su polimorfismo convierten a estos genes en un factor fundamental en la terapia con trasplantes, siendo su importancia máxima en los trasplantes de células progenitoras hematopoyéticas. Consecuentemente, la tipificación de estos antígenos en los estudios de compatibilidad ha sido desarrollada de manera paralela y en las últimas décadas se ha avanzado grandemente en su comprensión y caracterización. Varias metodologías moleculares son las que predominan actualmente para la tipificación de los antígenos de histocompatibilidad leucocitarios. La información obtenida de estas caracterizaciones ha permitido la aparición de bancos de donantes de células madre y unidades de cordón umbilical, los cuales amplían la probabilidad de encontrar un donador compatible para el paciente. Los programas de trasplante de células madre hematopoyéticas en nuestro país requieren de un avance en las tecnologías disponibles para tipificación de estas moléculas, así como de la instauración de un registro nacional de donantes basado en su tipificación molecular. El presente trabajo tiene por objetivo presentar el estado del conocimiento actual sobre los antígenos leucocitarios humanos, su genética, su tipificación, sus utilidades y protocolos a seguir en la tecnología de los transplantes de células madre.

The Human Leukocyte Antigen genetic system is the most polymorphic in humans. It plays a central role on immune response regulation by its interaction with molecules like the T-cellreceptor, participating in the antigen presentation process and self-recognition. This role addedto its polymorphism make the human leukocyte antigens a fundamental factor for transplantation, especially when it comes to hematopoietic stem cell transplants. Consequently, techniques for human leukocyte antigen typing for compatibility studies have experienced great development over the last decades. Various molecular typing methodologies currently predominate for this characterization. Information obtained with these technologies has prompted the development of stem cell adult donor registries and cord blood banks which raise the probability of finding a suitable compatible donor for patients in need of transplantation. Stem Cell Transplantation Programs in Costa Rica urgently need the updating to molecular typing technologies for patientdonor compatibility studies. Moreover, the creation of a National Stem Cell Donor Registry and the pursuing of the public Cord Blood Bank need to be addressed. The present review aims to present state-of-the-art concepts and knowledge on human leukocyte antigen genetics, typingstrategies and protocols, and applications on stem cell transplantation. Additionally, perspectives for Costa Rican development on these areas are given.

Frecuencias alélicas, genotípicas y haplotípicas HLA-A, HLA-B, HLA-DRB1 en donantes fallecidos, Medellín, Colombia / Human leucocyte antigen gene (HLA-A, HLA-B, HLA-DRB1) frequencies in deceased organ donors

Introducción. La caracterización genética del sistema HLA es de gran utilidad en estudios antropogenéticos, en la comprensión de mecanismos asociados a susceptibilidad o resistencia a diversas enfermedades, en los fenómenos inmunológicos durante el embarazo y en la selección de donantes/receptores en trasplantes de órganos. Objetivo. Determinar las frecuencias alélicas, genotípicas y haplotípicas HLA-A, -B, -DRB1 en donantes fallecidos en Medellín. Materiales y métodos. Se incluyeron 926 donantes entre febrero de 1989 y septiembre de 2006, a los cuales se les realizó la tipificación HLA-A, -B, -DRB1 por PCR-SSP (single specific primer-polymerase chain reaction) de mediana resolución. Las frecuencias alélicas, genotípicas y haplotípicas fueron estimadas mediante el algoritmo de máxima verosimilitud. Se evaluó el ajuste al equilibrio de Hardy-Weimberg por una prueba exacta análoga a la de Fisher usando la cadena de Markov, así como el desequilibrio de ligamiento entre pares de loci. Resultados. Se identificaron 22, 43 y 14 alelos para los loci HLA-A, -B, -DRB, respectivamente, de los cuales los más frecuentes fueron: A*02, A*24, B*35 y DRB1*04. En los loci HLA-A y -B se observó deficiencia en la frecuencia de heterocigóticos esperada (p<0,01 y p<0,00001, respectivamente). Los haplotipos más frecuentes fueron HLA-A*24, B*35 (7,7 por ciento), HLA-B*35 DRB1*04 (6,4 por ciento) y HLA-A*24, DRB1*04 (8,9 por ciento) para HLA-A, -DRB1, y para 3 loci fueron HLA-A*24, B*35, DRB1*04 (4,6 por ciento) y HLA-A*24, B*61, DRB1*04 (2,0 por ciento). Conclusiones. Estos resultados corroboran la composición triétnica de nuestra población, en la cual predomina el grado de mezcla caucásica, a diferencia de otras latinoamericanas, y podrán ser usados como referencia para otros estudios y aplicaciones en esta población.

Introduction. Genetic characterization of the human leucocyte antigen (HLA) system has provided insights into mechanisms of susceptibility to diverse diseases and immunological phenomena during pregnancy, as well as providing evidence for compatibility in the selection of organ transplant donors and recipients. Objective. The HLA-A,-B,-DRB1 allele, genotype and haplotype frequencies were determined in deceased organ donors in Medellín, Colombia. Materials and methods. The genotypes of 926 deceased donors were evaluated over a 17-year period (1989- 2006). HLA-A, HLA-B and HLA-DRB1 typing was performed by sequence specific primer-polymerase chain reaction (SSP-PCR). Maximum likelihood frequencies were estimated by the zipper version of expectation maximation algorithm. Hardy-Weinberg equilibrium were determined by an exact test analogous to Fisher’s test by using Markov’s chain, and linkage disequilibrium between pairs of loci. Results. Twenty-two, 43 and 14 alleles were identified for HLA-A, -B and -DRB loci, respectively. The most frequent were A*02, A*24, B*35, and DRB1*04. A deficiency in the proportion of heterozygotes in HLA-A and B loci (p<0.01 and p<0.00001, respectively). The most frequent haplotypes were as follows: HLA-A*24, B*35 (7.7%) for HLA-A,-B; HLA-B*35, DRB1*04 (6.4%) for HLA-B,-DRB1 and HLA-A*24, DRB1*04 (8.9%) for HLA-A,-DRB1. For the 3 loci HLA-A,-B,-DRB1, the most frequent haplotypes were A*24, B*35, DRB1*04 (4.6%) and A*24, B*61,DRB1*04 (2.0%). Conclusions. These results confirm the three-ethnic ancestry of the Medellin population. The predominance of Caucasian admixture differs from many other Latin-American populations and can serve as a reference for comparative studies of these populations as well as applications within the Medellin population.

Allogeneic hematopoietic stem cell transplantation from an alternative stem cell source in Fanconi anemia patients: analysis of 47 patients from a single institution

We transplanted 47 patients with Fanconi anemia using an alternative source of hematopoietic cells. The patients were assigned to the following groups: group 1, unrelated bone marrow (N = 15); group 2, unrelated cord blood (N = 17), and group 3, related non-sibling bone marrow (N = 15). Twenty-four patients (51 percent) had complete engraftment, which was not influenced by gender (P = 0.87), age (P = 0.45), dose of cyclophosphamide (P = 0.80), nucleated cell dose infused (P = 0.60), or use of anti-T serotherapy (P = 0.20). Favorable factors for superior engraftment were full HLA compatibility (independent of the source of cells; P = 0.007) and use of a fludarabine-based conditioning regimen (P = 0.046). Unfavorable factors were > or = 25 transfusions pre-transplant (P = 0.011) and degree of HLA disparity (P = 0.007). Intensity of mucositis (P = 0.50) and use of androgen prior to transplant had no influence on survival (P = 0.80). Acute graft-versus-host disease (GVHD) grade II-IV and chronic GVHD were diagnosed in 47 and 23 percent of available patients, respectively, and infections prevailed as the main cause of death, associated or not with GVHD. Eighteen patients are alive, the Kaplan-Meyer overall survival is 38 percent at ~8 years, and the best results were obtained with related non-sibling bone marrow patients. Three recommendations emerged from the present study: fludarabine as part of conditioning, transplant in patients with <25 transfusions and avoidance of HLA disparity. In addition, an extended family search (even when consanguinity is not present) seeking for a related non-sibling donor is highly recommended.

Association of HLA phenotype with primary non-response to recombinant hepatitis B vaccine: a study from north India.

The hepatitis B vaccine is considered to be highly immunogenic and has a good safety profile. In adults, it has a primary non-response rate of 5%-10%. Causes of nonresponse to hepatitis B vaccine include age, sex, obesity smoking. Certain human leucocyte antigen (HLA) phenotypes have been known to be associated with responsiveness to the vaccine, and found to be different in different ethnic groups, such as Caucasians and Orientals. The study was designed to identify the HLA phenotypes that are associated with non-responsiveness to hepatitis B virus (HBV) vaccination amongst a cohort of Indian subjects who agreed to participate in the vaccination programme. The study was offered to 107 volunteers, of whom 102 were found to be negative for HBV markers (hepatitis B surface antigen [HBsAg], anti-HBc, anti-HBe, anti-HBs, hepatitis Be antigen [HBeAg]) . All 102 volunteers were offered recombinant hepatitis B vaccine (20 microg) at 0, 1, and 6 months. Anti-HBs antibody titres were tested on days 90 and 210 of the first vaccine dose. HLA typing was done using standard microlymphotoxicity tests. The seroconversion rate of the hepatitis B vaccine was 86.3% (88/102). Fifteen nonresponders (15/102) and 15 of the 88 responders were randomly selected after age and sex matching for the purpose of studying the HLA phenotypes. HLA subtypes A1, B15, B40, A10 and DQ2 were found to be increased among nonresponders while HLA- A11, C3, DR10, DR51 (p>0.05) were the most common phenotypes amongst the responders. Further studies are needed to characterize the HLA phenotypes amongst the responders in different ethnic groups in India with respect to HBV vaccination.

HLA expression in aortic and pulmonary homografts: effects of cryopreservation.

BACKGROUND: The present study was undertaken to find out the HLA allo-antigens on cardiac homografts. METHODS AND RESULTS: One pulmonary and eight aortic homografts were studied for the presence of major HLA class I and class II antigen expression. Cadaveric hearts were procured from the mortuary and kept in Hank's balanced salt solution with antibiotics at 4 degrees C. Bits were taken from the conduits and valves every 24 hours for 14 days during storage and snap-frozen using liquid nitrogen. A total of 1368 sections were made using a cryostat. These sections were stained using 4 monoclonal antibodies: BLA class I (MO736), class II HLA-DR (MO746), CD45 (MO701), and endothelial stain (MO616). All monoclonals were procured from DAKO. Class I antigen molecules could be demonstrated on the endothelial surface of the vessel wall from day 1 to day 4 to 5 of storage. They stained weaker and could not be demonstrated after day 10 of storage. Class I antigen molecules were positive in very fresh valves and by day 5-6 could not be seen on the valve surface. Class II (HLA-DR) antigen expression was present in the subendothelial layer from day 1 to day 12-14 of storage. They could also be demonstrated in valves and conduits released after cryopreservation. These class II staining cells were also stained by CD45 monoclonal antibody and hence could be macrophages, histiocytes or leucocytes. The endothelium was very well demonstrated in the vessel walls from day 1 to day 12-14 of storage; it could only be seen in very fresh valves. Storage in the liquid medium and sterilization procedures led to loss of endothelial lining of the valves. After cryopreservation and thawing, class I antigen molecules could not be demonstrated on the valves and conduits. Class II antigen molecules and CD45-stained cells continued to be demonstrated in the subendothelial layer and the valve matrix. The endothelium was intact in the vessel wall after cryopreservation and thawing, but could not be seen in the released valves. CONCLUSIONS: Allograft aortic and pulmonary conduits and valves are immunogenic, and HLA-ABC and HLA-DR antigen molecules can be demonstrated on different components of the vessel wall and valve leafets.

Prevalência de alterações tireoidianas em funcionários da UFRJ e estudo imunogenético anti-tireoidianos positivos / Prevalence of thyroid disorders and imunogenetc study in workers from UFRJ with positive ATPO

Os objetivos da pesquisa foram verificar a prevalência de desordens tireoidianas como bócio, disfunção e anticorpos anti-TPO positivos na população de funcionários da UFRJ e comparar as frequências dos alelos HLA DRB1 e DQB1 entre pacientes com anticorpos positivos e pessoas sadias sem história familiar de doenças auto-imunes. Em todos os 302 indivíduos selecionados por amostragem aleatória simples (210 mulheres e 93 homens, com média de idade de 43,5 e 43 anos, respectivamente) foi feito ratreamento com avaliação clínica, dosagem de TSH e de anticorpos anti-TPO. Quando necessário, outros exames foram realizados como complemento diagnóstico. A tipagem HLA realizada com placas para os alelos DRB1 e DQB1 genéricos utilizou a técnica de SSP baseada na PCR. Alterações à palpação da tireóide foram encontradas em 38 pessoas (12,6 por cento) e em mais 44 a glândula era visível (14,6 por cento), sem diferença significativa entre as frequências nos dois sexos. Vinte e oito (9,3 por cento) tinham anticorpo anti-TPO positivo, com prevalência de 10 por cento, nas mulheres e 7,6 por cento nos homens. Alterações do TSH foram encontradas em 7,3 por cento, sendo TSH baixo em 4 por cento e TSH alto em 3,3 por cento. Em quase todas as comparações, as desordens foram mais prevalentes em pessoas a partir dos 40 anos. Entre os alelos DRB1, o *1131 só foi encontrado em controles (pcorr < 0,05). Para todos os alelos não foram encontrados frequências significativamente diferentes entre os dois grupos. Os resultados da invstigação epidemiológica foram semelhantes aos de outors estudos para algumas alterações, geralmente mais prevalentes em mulheres e a partir dos 40 anos. Entretanto, a prevalência de anticoropos positivos nos homens foi mairo do que o esperado. Os resultados do estudo imunogenético não permitem conclusões definitivas em relação à associação do HLA com doenças auto-imunes da tireóide

Alterations of HLA class I and II antigen expression in preinvasive, invasive and metastatic cervical cancers

HLA expression is altered in a large variety of human cancers. We performed immunohistochemical staining on tissues from normal, preinvasive, invasive and metastatic cervical cancer tissues using anti-HLA class I or class II antibody. In tissues from normal squamous epithelium, carcinoma in situ (CIS) and microinvasive carcinoma (MIC), the expressions of HLA-B, C heavy chains and class II heavy chain were significantly decreased as disease progressed. When the expression patterns were compared between primary and metastatic squamous cell carcinoma (SCC) lesions, statistically significant down-regulation of HLA class I and class II antigen in metastatic lesions was observed. The rates of HLA-B, C heavy chains and class II heavy chain expressions were all significantly down-regulated compared to the down-regulation rate of class I beta2-microglobulin (beta2m) in invasive squamous lesions, and the expressions of class II heavy chain in metastatic lesions was decreased further than that in primary lesions. Unlike SCC, the degree of HLA class I and class II loss was not evident as disease progressed in early stage of adenocarcinoma. In invasive adenocarcinoma lesions, only the expression of HLA-B, C heavy chains was decreased and no differences were seen in HLA-B, C heavy chain expression patterns between primary and metastatic lesions. These results suggest that alterations of HLA class I and II expressions seem to occur at a particular step in cervical cancer development and depend on tissue types: when the tumor becomes invasive and starts to metastasize.

Preliminary study of HLA-ABCDR antigens in CML, ANLL, thalassemia and severe aplastic anemia in Thais.

The objective of this study was to analyse human leukocyte antigen (HLA) and disease association in common blood diseases [chronic myelogenous leukemia (CML), acute nonlymphocytic leukemia (ANLL), thalassemia and severe aplastic anemia] in Thais. The subjects were patients from the Hematological Clinic, Departments of Medicine and Pediatrics, Ramathibodi Hospital who were referred for HLA typing for bone marrow transplantation (BMT) at the Histocompatibility Laboratory from March 1988 to September 1997. A total of 129 patients had complete HLA-ABC typing. The patients included 45 CML, 40 ANLL, 26 thalassemia (Thal) and 18 severe aplastic anemia (SAA). Of these, 88 patients were typed for HLA class II. The HLA class I (ABC) and II (DR, DQ) typings were performed by microlymphocytotoxicity test. It was found that HLA class I was associated with CML, ANLL and Thal, whereas, HLA class II was associated with SAA. HLA-B8 and HLA-B18 were increased in CML with R.R. values of 12.2 and 3.9, respectively, whereas, HLA-B18 was increased in ANLL with R.R. value of 4.5. In addition, HLA-DR2 and DR3 were increased in SAA with R.R. values of 3.8 and 4.8, respectively. For Thal, HLA-A2 and B46 were increased in Thal in Central Thais with R.R. values of 3.3 and 6.1, respectively, whereas, HLA-B13 was increased in Thal in Northern Thais with R.R. value of 8.5. On the other hand, HLA-B7 was absent in CML. HLA-Cw7 was decreased in CML and SAA, whereas, HLA-DR6 was decreased in ANLL and SAA. Furthermore, HLA-Cw6 was also decreased in CML, whereas, HLA-A33 and Bw4 were decreased in SAA. Although the sample size of each disease was small, the increase of HLA-DR2 was observed in SAA in Thais which was similar to other studies in different ethnic groups. These preliminary data may be useful for further study in HLA and blood disease association.

Perfil inmunologico del paciente con trasplante renal en Panama / Immunologic profile of patients with renal transplantation in Panama

We are presenting the immunologic pattern of 100 patients with kidney transplant made from 1990-2000 at CHM CSS Dr.AAM. Eighty nine were alive related donors. Most of them were from blood group O, donors and receptors. They came from Panama, Chiriqui and Colon. Many of the donors were siblings. The grades of compatibility in frequency were D, C, A & B. For locus HLA-A the most common gen was A2 for transplanted patients and for the rest of the Panamanian population is A24. For the locus HLA-B were B35 and B38 respectively and for the locus HLA-C the most common gen was C4, and C3 for the rest of the population